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狼疮性肾炎患者中诱导致病性自身抗体的γ/δ辅助性T细胞表达异常的T细胞受体。

Pathogenic autoantibody-inducing gamma/delta T helper cells from patients with lupus nephritis express unusual T cell receptors.

作者信息

Rajagopalan S, Mao C, Datta S K

机构信息

Department of Medicine, New England Medical Center, Boston, Massachusetts 02111.

出版信息

Clin Immunol Immunopathol. 1992 Mar;62(3):344-50. doi: 10.1016/0090-1229(92)90113-3.

DOI:10.1016/0090-1229(92)90113-3
PMID:1531788
Abstract

In previous work, we found that only 59 (15%) of 396 "autoreactive" T cell clones derived from five patients with lupus nephritis had the ability to selectively augment the production of pathogenic anti-DNA autoantibodies and the majority (49/59) of those autoimmune T helper (Th) clones were CD4+. Surprisingly, 7 of those Th clones were CD4-/CD8- and gamma/delta TCR+, capable of augmenting the production of pathogenic anti-DNA autoantibodies up to 125-fold. The gamma/delta Th clones responded in a MHC-nonrestricted manner to some endogenous autoantigen associated with heat shock proteins (HSP60) on the lupus B cells. The gamma/delta TCR genes expressed by 4 of these Th clones were amplified and sequenced here. Three of the 4 Th clones, each from a different lupus patient, expressed a gene from the V gamma 1 subgroup. Moreover, 2 of the Th clones expressed V delta 5, and the others V delta 1 or V delta 3. These TCRs are rarely expressed by peripheral blood gamma/delta T cells of normal adult humans. The predominant gamma/delta T cells in human peripheral blood express V gamma 2 (V gamma 9) and V delta 2 TCR genes, including HSP-responsive T cells. None of the lupus Th clones expressed this combination of TCR genes. In addition, some of these pathogenic autoantibody-inducing Th clones from the lupus patients had limited diversity and few N-nucleotide additions in their gamma/delta TCR junctional regions (CDR3), thus resembling fetal gamma/delta thymocytes early in ontogeny.

摘要

在之前的研究中,我们发现,从5名狼疮性肾炎患者中获得的396个“自身反应性”T细胞克隆中,只有59个(15%)能够选择性地增强致病性抗DNA自身抗体的产生,并且这些自身免疫性辅助性T(Th)细胞克隆中的大多数(49/59)是CD4+。令人惊讶的是,其中7个Th细胞克隆是CD4-/CD8-且γ/δTCR+,能够将致病性抗DNA自身抗体的产生增强至125倍。这些γ/δTh细胞克隆以MHC非限制性方式对狼疮B细胞上一些与热休克蛋白(HSP60)相关的内源性自身抗原作出反应。这里对其中4个Th细胞克隆表达的γ/δTCR基因进行了扩增和测序。这4个Th细胞克隆中的3个,每个都来自不同的狼疮患者,表达了Vγ1亚组的一个基因。此外,2个Th细胞克隆表达Vδ5,其他的表达Vδ1或Vδ3。正常成年人外周血γ/δT细胞很少表达这些TCR。人类外周血中占主导的γ/δT细胞表达Vγ2(Vγ9)和Vδ2 TCR基因,包括对HSP有反应的T细胞。狼疮患者的这些致病性自身抗体诱导性Th细胞克隆均未表达这种TCR基因组合。此外,狼疮患者中一些诱导致病性自身抗体的Th细胞克隆在其γ/δTCR连接区(CDR3)的多样性有限且N核苷酸添加很少,因此类似于个体发育早期的胎儿γ/δ胸腺细胞。

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Pathogenic autoantibody-inducing gamma/delta T helper cells from patients with lupus nephritis express unusual T cell receptors.狼疮性肾炎患者中诱导致病性自身抗体的γ/δ辅助性T细胞表达异常的T细胞受体。
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Nucleosome: a major immunogen for pathogenic autoantibody-inducing T cells of lupus.核小体:狼疮致病性自身抗体诱导性T细胞的主要免疫原。
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Gamma delta T-cell help in responses to pathogens and in the development of systemic autoimmunity.
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